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COVID-19 has emerged, and has rapidly become a major health problem worldwide, causing millions of mortalities. Vaccination against COVID-19 is the most efficient way to stop the pandemic. The goal of vaccines is to induce neutralizing antibodies against SARS-CoV-2 virus. Here, we present a novel double mosaic virus-like particle (VLP) displaying two independent neutralizing epitopes, namely the receptor binding motif (RBM) located in S1 and the fusion peptide (AA 817–855) located in S2. CuMV_TT virus-like particles were used as VLP scaffold and both domains were genetically fused in the middle of CuMV_TT subunits, which co-assembled into double mosaic particles (CuMV_TT-DF). A single fusion mosaic particle (CuMV_TT-FP) containing the fusion peptide only was used for comparison. The vaccines were produced in E. coli, and electron microscopy and dynamic light scattering confirmed their integrity and homogeneity. In addition, the CuMV_TT-DF vaccine was well recognized by ACE2 receptor, indicating that the RBM was in native conformation. Both CuMV_TT-FP and CuMV_TT-DF vaccines induced high levels of high avidity IgG antibodies as well as IgA recognizing spike and RBD in the case of CuMV_TT-DF. Both vaccine candidates induced virus-neutralizing antibodies indicating that the fusion peptide can independently induce virus-neutralizing antibodies. In contrast, CuMV_TT-DF containing both RBM and fusion peptide induced a higher level of neutralizing antibodies suggesting that the new double mosaic vaccine candidate CuMV_TT-DF consisting of two antigens in one VLP maybe an attractive candidate for scale-up in a …